| Literature DB >> 32135573 |
Roger Hudson1,2, Matthew Green1,2, Daniel J Wright1,2, Justine Renard1,2, Christina E L Jobson1,2, Tony Jung1,2, Walter Rushlow1,2,3, Steven R Laviolette1,2,3.
Abstract
Long-term tobacco dependence typically develops during adolescence and neurodevelopmental nicotine exposure is associated with affective disturbances that manifest as a variety of neuropsychiatric comorbidities in clinical and preclinical studies, including mood and anxiety-related disorders. The nucleus accumbens shell (NASh) is critically involved in regulating emotional processing, and both molecular and neuronal disturbances in this structure are associated with mood and anxiety-related pathologies. In the present study, we used a rodent model of adolescent neurodevelopmental nicotine exposure to examine the expression of several molecular biomarkers associated with mood/anxiety-related phenotypes. We report that nicotine exposure during adolescence (but not adulthood) induces profound upregulation of the ERK 1-2 and Akt-GSK-3 signalling pathways directly within the NASh, as well as downregulation of local D1R expression that persists into adulthood. These adaptations were accompanied by decreases in τ, α, β, and γ-band oscillatory states, hyperactive medium spiny neuron activity with depressed bursting rates, and anxiety and depressive-like behavioural abnormalities. Pharmacologically targeting these molecular and neuronal adaptations revealed that selective inhibition of local ERK 1-2 and Akt-GSK-3 signalling cascades rescued nicotine-induced high-γ-band oscillatory signatures and phasic bursting rates in the NASh, suggesting that they are involved in mediating adolescent nicotine-induced depressive and anxiety-like neuropathological trajectories.Entities:
Keywords: GSK-3; adolescence; anxiety; nicotine; nucleus accumbens; oscillations
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Year: 2020 PMID: 32135573 DOI: 10.1111/adb.12891
Source DB: PubMed Journal: Addict Biol ISSN: 1355-6215 Impact factor: 4.280